首页> 外文期刊>Journal of neurology >Intrathecal anti-alphaB-crystallin IgG antibody responses: potential inflammatory markers in Guillain-Barre syndrome.
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Intrathecal anti-alphaB-crystallin IgG antibody responses: potential inflammatory markers in Guillain-Barre syndrome.

机译:鞘内抗αB-晶状体IgG抗体反应:格林-巴利综合征中潜在的炎症标志物。

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OBJECTIVE: alphaB-crystallin (alphaBC), a small stress protein with cytoprotective and anti-apoptotic functions, is a potent antigen in autoimmune demyelinating diseases. To address the role of alphaBC in Guillain-Barre syndrome (GBS) we analyzed humoral responses against alphaBC in relation to clinical, electrophysiological and CSF features in GBS. METHODS: Anti-alphaBC-IgG antibodies were measured in serum and cerebrospinal fluid (CSF) of patients with GBS (n = 41), infectious inflammatory neurological diseases (n = 21), multiple sclerosis (n = 42), and other, non-inflammatory neurological disorders (n = 40) by ELISA using human recombinant alphaBC. Expression of alphaBC was immunohistochemically analyzed in postmortem peripheral nerve tissue of GBS and controls without neuropathy. RESULTS: Serum alphaBC-IgG antibody levels did not differ between disease groups, whereas alphaBC-IgG antibodies in CSF were increased in GBS and infectious inflammatory neurological diseases. Calculation of an antigen specific alphaBC-IgG index (alphaBC-Ig-G(CSF) x total IgG(CSF))/(alphaBC-IgG(Serum) x total IgG(Serum)) revealed significantly elevated values in patients with GBS compared to other disease groups (p < 0.001). alphaBC-IgG indices exceeding a cut off value > 0.8 had an 85 % specificity and a 76 % sensitivity for GBS. alphaBC was overexpressed in dorsal root ganglia and spinal roots of autopsy cases with GBS. CONCLUSIONS: We demonstrate increased alphaBC-IgG indices in a high proportion of our GBS patients, which reflect enhanced antigen-specific intrathecal antibody responses against abnormally expressed alphaBC in inflamed peripheral nerve tissue. Elevated alphaBC-IgG indices might therefore serve as markers of PNS inflammation and supplement currently used laboratory tests in the diagnosis of GBS.
机译:目的:αB-晶状体蛋白(alphaB-crystallin,一种具有细胞保护和抗凋亡功能的应激蛋白)是自身免疫性脱髓鞘疾病的有效抗原。为了解决alphaBC在格林巴利综合征(GBS)中的作用,我们分析了针对alphaBC的体液反应,涉及GBS的临床,电生理和脑脊液特征。方法:对GBS(n = 41),传染性炎性神经系统疾病(n = 21),多发性硬化症(n = 42)和其他非血清的患者的血清和脑脊液(CSF)进行抗αBC-IgG抗体检测使用人重组alphaBC的ELISA检测-炎症性神经系统疾病(n = 40)。免疫组化分析了GBS的死后外周神经组织和无神经病变的对照组中alphaBC的表达。结果:疾病组之间的血清αBC-IgG抗体水平没有差异,而GBS和传染性炎性神经疾病中CSF中的αBC-IgG抗体升高。抗原特异性alphaBC-IgG指数(alphaBC-Ig-G(CSF)x总IgG(CSF))/(alphaBC-IgG(Serum)x总IgG(Serum))的计算显示,与之相比,GBS患者的值显着升高其他疾病组(p <0.001)。超过临界值> 0.8的alphaBC-IgG指数对GBS的特异性为85%,敏感性为76%。在患有GBS的尸检病例的背根神经节和脊神经根中过表达alphaBC。结论:我们证明了我们的GBS患者中有很大比例的alphaBC-IgG指数升高,这反映了针对发炎的周围神经组织中异常表达的alphaBC的抗原特异性鞘内抗体反应增强。因此,升高的alphaBC-IgG指数可能会成为PNS炎症的标志物,并补充当前用于诊断GBS的实验室测试。

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